Your search keyword '"Curtis A. Engelhart"' showing total 4 results

1. Optimization of TAM16, a Benzofuran That Inhibits the Thioesterase Activity of Pks13; Evaluation toward a Preclinical Candidate for a Novel Antituberculosis Clinical Target

Author

Caroline Wilson, Peter Ray, Fabio Zuccotto, Jorge Hernandez, Anup Aggarwal, Claire Mackenzie, Nicola Caldwell, Malcolm Taylor, Margaret Huggett, Michael Mathieson, Dinakaran Murugesan, Alasdair Smith, Susan Davis, Mattia Cocco, Maloy K. Parai, Arjun Acharya, Fabio Tamaki, Paul Scullion, Ola Epemolu, Jennifer Riley, Laste Stojanovski, Eva Maria Lopez-Román, Pedro Alfonso Torres-Gómez, Ana Maria Toledo, Laura Guijarro-Lopez, Isabel Camino, Curtis A. Engelhart, Dirk Schnappinger, Lisa M. Massoudi, Anne Lenaerts, Gregory T. Robertson, Chris Walpole, David Matthews, David Floyd, James C. Sacchettini, Kevin D. Read, Lourdes Encinas, Robert H. Bates, Simon R. Green, and Paul G. Wyatt

Subjects

Models, Molecular, 0303 health sciences, ERG1 Potassium Channel, 010405 organic chemistry, Antitubercular Agents, Heart, Microbial Sensitivity Tests, Mycobacterium tuberculosis, 01 natural sciences, Cardiotoxicity, Article, 0104 chemical sciences, 3. Good health, 03 medical and health sciences, Structure-Activity Relationship, Bacterial Proteins, Palmitoyl-CoA Hydrolase, Piperidines, Drug Discovery, Molecular Medicine, Humans, Polyketide Synthases, 030304 developmental biology, Benzofurans

Abstract

With increasing drug resistance in tuberculosis (TB) patient populations, there is an urgent need for new drugs. Ideally, new agents should work through novel targets so that they are unencumbered by preexisting clinical resistance to current treatments. Benzofuran 1 was identified as a potential lead for TB inhibiting a novel target, the thioesterase domain of Pks13. Although, having promising activity against Mycobacterium tuberculosis, its main liability was inhibition of the hERG cardiac ion channel. This article describes the optimization of the series toward a preclinical candidate. Despite improvements in the hERG liability in vitro, when new compounds were assessed in ex vivo cardiotoxicity models, they still induced cardiac irregularities. Further series development was stopped because of concerns around an insufficient safety window. However, the demonstration of in vivo activity for multiple series members further validates Pks13 as an attractive novel target for antitubercular drugs and supports development of alternative chemotypes.

Published

2021

2. Antitubercular 2-Pyrazolylpyrimidinones: Structure-Activity Relationship and Mode-of-Action Studies

Author

Kirsteen I. Buchanan, Clifton E. Barry, Simon Green, Gregory S. Basarab, Qin Su, Charles J. Eyermann, Curtis A. Engelhart, Anuradha Kumar, Paul D. van Helden, Frederick A. Sirgel, Paul G. Wyatt, Nina Lawrence, Sandeep R. Ghorpade, Dirk Schnappinger, Dale Taylor, Sandile B. Simelane, Helena I. Boshoff, Christel Brunschwig, Vinayak Singh, Kelly Chibale, Peter C. Ray, Tracy Bayliss, Candice Soares de Melo, Alissa Myrick, Tanya Parish, and Timothy G. Myers

Subjects

Male, Phenotypic screening, Iron, Mutant, Antitubercular Agents, Microbial Sensitivity Tests, Pyrimidinones, 01 natural sciences, Article, Mycobacterium tuberculosis, 03 medical and health sciences, Minimum inhibitory concentration, Mice, Structure-Activity Relationship, Bacterial Proteins, Microsomes, Drug Discovery, medicine, Structure–activity relationship, Animals, Humans, Mode of action, 030304 developmental biology, 0303 health sciences, biology, Chemistry, Membrane Transport Proteins, biology.organism_classification, In vitro, 0104 chemical sciences, Rats, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, Biochemistry, Mechanism of action, Mutation, Molecular Medicine, Pyrazoles, medicine.symptom, Half-Life

Abstract

Phenotypic screening of a Medicines for Malaria Venture compound library against Mycobacterium tuberculosis (Mtb) identified a cluster of pan-active 2-pyrazolylpyrimidinones. The biology triage of these actives using various tool strains of Mtb suggested a novel mechanism of action. The compounds were bactericidal against replicating Mtb and retained potency against clinical isolates of Mtb. Although selected MmpL3 mutant strains of Mtb showed resistance to these compounds, there was no shift in the minimum inhibitory concentration (MIC) against a mmpL3 hypomorph, suggesting mutations in MmpL3 as a possible resistance mechanism for the compounds but not necessarily as the target. RNA transcriptional profiling and the checkerboard board 2D-MIC assay in the presence of varying concentrations of ferrous salt indicated perturbation of the Fe-homeostasis by the compounds. Structure-activity relationship studies identified potent compounds with good physicochemical properties and in vitro microsomal metabolic stability with moderate selectivity over cytotoxicity against mammalian cell lines.

Published

2021

3. Discovery and Structure-Activity-Relationship Study of N-Alkyl-5-hydroxypyrimidinone Carboxamides as Novel Antitubercular Agents Targeting Decaprenylphosphoryl-β-d-ribose 2'-Oxidase

Author

Sangmi, Oh, Yumi, Park, Curtis A, Engelhart, Joshua B, Wallach, Dirk, Schnappinger, Kriti, Arora, Michelle, Manikkam, Brian, Gac, Hongwu, Wang, Nicholas, Murgolo, David B, Olsen, Michael, Goodwin, Michelle, Sutphin, Danielle M, Weiner, Laura E, Via, Helena I M, Boshoff, and Clifton E, Barry

Subjects

Alkylation, Protein Conformation, Antitubercular Agents, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Pyrimidinones, Article, High-Throughput Screening Assays, Molecular Docking Simulation, Mice, Structure-Activity Relationship, Drug Design, Animals, Female, Tissue Distribution, Molecular Targeted Therapy, Oxidoreductases

Abstract

Magnesium plays an important role in infection with Mycobacterium tuberculosis ( Mtb) as a signal of the extracellular environment, as a cofactor for many enzymes, and as a structural element in important macromolecules. Raltegravir, an antiretroviral drug that inhibits HIV-1 integrase is known to derive its potency from selective sequestration of active-site magnesium ions in addition to binding to a hydrophobic pocket. In order to determine if essential Mtb-related phosphoryl transfers could be disrupted in a similar manner, a directed screen of known molecules with integrase inhibitor-like pharmacophores ( N-alkyl-5-hydroxypyrimidinone carboxamides) was performed. Initial hits afforded compounds with low-micromolar potency against Mtb, acceptable cytotoxicity and PK characteristics, and robust SAR. Elucidation of the target of these compounds revealed that they lacked magnesium dependence and instead disappointingly inhibited a known promiscuous target in Mtb, decaprenylphosphoryl-β-d-ribose 2'-oxidase (DprE1, Rv3790).

Published

2018

4. Non-Nucleoside Inhibitors of BasE, an Adenylating Enzyme in the Siderophore Biosynthetic Pathway of the Opportunistic Pathogen Acinetobacter baumannii

Author

Daniel J. Wilson, Curtis A. Engelhart, Eric J. Drake, rd Clifton E. Barry, Andrew M. Gulick, Courtney C. Aldrich, Helena I. Boshoff, João Neres, and Peng Fu

Subjects

Acinetobacter baumannii, Models, Molecular, Siderophore, Protein Conformation, Klebsiella pneumoniae, Siderophores, Virulence, Microbial Sensitivity Tests, medicine.disease_cause, Article, Microbiology, Structure-Activity Relationship, Drug Discovery, medicine, Enzyme Inhibitors, Escherichia coli, chemistry.chemical_classification, biology, Pseudomonas aeruginosa, biology.organism_classification, Anti-Bacterial Agents, Enzyme, Biochemistry, chemistry, Molecular Medicine, Bacteria

Abstract

Siderophores are small-molecule iron chelators produced by bacteria and other microorganisms for survival under iron limiting conditions such as found in a mammalian host. Siderophore biosynthesis is essential for the virulence of many important Gram-negative pathogens including Acinetobacter baumannii, Klebsiella pneumoniae, Pseudomonas aeruginosa, and Escherichia coli. We performed high-throughput screening against BasE, which is involved in siderophore biosynthesis in A. baumannii, and identified 6-phenyl-1-(pyridin-4-ylmethyl)-1H-pyrazolo[3,4-b]pyridine-4-carboxylic acid 15. Herein we report the synthesis, biochemical, and microbiological evaluation of a systematic series of analogues of the HTS hit 15. Analogue 67 is the most potent analogue with a KD of 2 nM against BasE. Structural characterization of the inhibitors with BasE reveals that they bind in a unique orientation in the active site, occupying all three substrate binding sites, and thus can be considered as multisubstrate inhibitors. These results provide a foundation for future studies aimed at increasing both enzyme potency and antibacterial activity.

Published

2013